Gaoxin Zhang, Zelun Zhi, Bin Pan, Zemin Li, Shuyan Zhang, Zhenzhen Wu, Pengcheng Bu, Zhen Cao, Pingsheng Liu
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引用次数: 0
摘要
新甘壁酸(Neogambogic acid,NGA)是一种强效抗肿瘤药物,但在临床应用中却面临着极大的障碍,包括极差的水溶性和全身毒性。为了克服这些障碍,一种新开发的纳米粒子--脂肪体(由磷脂单层膜包裹的中性脂质核心组成)被用于递送 NGA。本研究构建了负载 NGA 的阳离子脂肪体(NGA-C-ADs),其中 NGA 被包裹在中性脂质核心中,并被磷脂和阳离子脂质包围。NGA-C-ADs 中的 NGA 浓度高达 1.0 mg mL-1,比单独在水缓冲液中的浓度高 2000 倍。此外,体外细胞测试表明,与游离 NGA 相比,NGA-C-ADs 对各种癌细胞株具有更高的细胞毒性。此外,体内抗肿瘤动物实验表明,NGA-C-ADs 能有效抑制皮下 CT26 肿瘤小鼠的肿瘤生长,还能抑制化学诱导的肝细胞癌,且对主要器官无明显毒性。这些研究结果表明,NGA-C-ADs 具有治疗多种癌症的潜力。
Cationic Adiposomes as a Delivery System for Neogambogic Acid for the Treatment of Multiple Cancers
Neogambogic acid (NGA) is a potent antitumor drug but faces significant obstacles to clinical application, including extremely poor water solubility and systemic toxicity. To overcome these obstacles, a newly developed nanoparticle, adiposome, that consists of a neutral lipid core wrapped with a phospholipid-monolayer membrane, is utilized for the delivery of NGA. In this study, NGA-loaded cationic adiposomes (NGA-C-ADs) are constructed in which NGA is encapsulated within the neutral lipid core and surrounded by phospholipids and a cationic lipid. The concentration of NGA in NGA-C-ADs achieved is as high as 1.0 mg mL−1, which is 2 000-fold higher than in aqueous buffer alone. Moreover, in vitro cell tests revealed that NGA-C-ADs exhibited higher cytotoxicity against various cancer cell lines compared to free NGA. In addition, in vivo anti-tumor animal studies demonstrate that NGA-C-ADs effectively inhibit tumor growth in subcutaneous CT26 tumor-bearing mice and also suppress chemically-induced hepatocellular carcinoma without obvious toxicity to major organs. These findings suggest that NGA-C-ADs hold promise as a potential treatment for multiple cancers.